Biosynthesis of hibarimicins. II. Elucidation of biosynthetic pathway by cosynthesis using blocked mutants.

نویسندگان

  • Takayuki Kajiura
  • Tamotsu Furumai
  • Yasuhiro Igarashi
  • Hiroshi Hori
  • Kazuaki Higashi
  • Tadayuki Ishiyama
  • Masakazu Uramoto
  • Yoshimasa Uehara
  • Toshikazu Oki
چکیده

The biosynthetic pathway of hibarimicin (HBM) was proposed on the basis of the experimental results obtained by using blocked mutants of Microbispora rosea subsp. hibaria TP-A0121, the HBM producer. In its biosynthesis, the oxidative coupling of the aromatic undecaketide unit generates a symmetrical aglycon HMP-Y1 (hibarimicin-mutant product Y1), which is oxidatively modified to hibarimicinone, the HBM aglycon. The following glycosylation of hibarimicinone gives rise to the HBM complex. We identified that HMP-Y1 prepared by methanolysis of HMP-Y6, a glycosylated metabolite from a blocked mutant, was the key intermediate: transformation of 13C-labeled HMP-Y1 to HBM B was confirmed by NMR measurements. Mutant strain produced another type of aglycon HMP-P1 in which the coupled polyketide units were intramolecularly bridged by the ether bond. This metabolite also arose by the spontaneous elimination of methanol molecule from hibarimicinone.

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عنوان ژورنال:
  • The Journal of antibiotics

دوره 55 1  شماره 

صفحات  -

تاریخ انتشار 2002